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Inhibition of viral suppressor of RNAi proteins by designer peptides protects from enteroviral infection in vivo

Immunity. 2021-10; 
Yuan Fang , Zezhong Liu , Yang Qiu , Jing Kong, Yuhong Fu, Yujie Liu , Chong Wang , Jia Quan , Qian Wang , Wei Xu , Lei Yin , Jie Cui , Yi Xu , Stephen Curry , Shibo Jiang , Lu Lu , Xi Zhou
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Peptide Synthesis Peptides R8 ({PEG2}RRRRRRRR), P1 ({PEG2}RRRRRRRRAISDLLAS), P2 ({PEG2}RRRRRRRREEVRQYCRDQ), FITC-R8, FITC-P1, and FITC-P2 were synthesized by GenScript Biochem with 95% purity Get A Quote

摘要

RNA interference (RNAi) is the major antiviral mechanism in plants and invertebrates, but the absence of detectable viral (v)siRNAs in mammalian cells upon viral infection has questioned the functional relevance of this pathway in mammalian immunity. We designed a series of peptides specifically targeting enterovirus A71 (EV-A71)-encoded protein 3A, a viral suppressor of RNAi (VSR). These peptides abrogated the VSR function of EV-A71 in infected cells and resulted in the accumulation of vsiRNAs and reduced viral replication. These vsiRNAs were functional, as evidenced by RISC-loading and silencing of target RNAs. The effects of VSR-targeting peptides (VTPs) on infection with EV-A71 as well as another enteroviru... More

关键词

EV-A71; HFMD; VSR; antiviral RNAi immunity; antiviral drug; enterovirus; hand-foot-and-mouth disease; peptide drug; viral suppressor of RNAi.